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Exploiting Oligo(amido amine) Backbones for the Multivalent Presentation of Coiled-Coil Peptides

机译:利用Oligo(酰胺基胺)骨架进行螺旋多肽的多价呈递

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摘要

The investigation of coiled coil formation for one mono- and two divalent peptide-polymer conjugates is presented. Through the assembly of the full conjugates on solid support, monodisperse sequence-defined conjugates are obtained with defined positions and distances between the peptide side chains along the polymeric backbone. A heteromeric peptide design was chosen, where peptide K is attached to the polymer backbone, and coiled-coil formation is only expected through complexation with the complementary peptide E. Indeed, the monovalent peptide K-polymer conjugate displays rapid coiled-coil formation when mixed with the complementary peptide E sequence. The divalent systems show intramolecular homomeric coiled-coil formation on the polymer backbone despite the peptide design. Interestingly, this intramolecular assembly undergoes a conformational rearrangement by the addition of the complementary peptide E leading to the formation of heteromeric coiled coil polymer aggregates. The polymer backbone acts as a template bringing the covalently bound peptide strands in close proximity to each other, increasing the local concentration and inducing the otherwise nonfavorable formation of intramolecular helical assemblies.
机译:提出了一种单价和两种二价肽-聚合物共轭物的卷曲卷曲形成的研究。通过将完整的缀合物组装在固体支持物上,获得了具有沿聚合物主链的肽侧链之间的限定位置和距离的单分散序列限定的缀合物。选择了异源肽设计,其中肽K连接到聚合物主链上,只有通过与互补肽E络合才能预期形成卷曲螺旋。确实,当混合时,单价肽K-聚合物偶联物显示出快速卷曲螺旋形成与互补的肽E序列。尽管有肽设计,二价体系仍在聚合物主链上显示出分子内同源的卷曲螺旋形成。有趣的是,该分子内组装体通过添加互补肽E而经历构象重排,导致形成异聚的卷曲螺旋聚合物聚集体。聚合物主链充当模板,使共价结合的肽链彼此紧邻,从而增加了局部浓度并诱导了分子内螺旋组装体的其他不利形成。

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